Latent TGF-β Activation Is a Hallmark of the Tenascin Family

Aubert, Alexandre; Mercier-Gouy, Perrine; Aguero, Stéphanie; Berthier, Laurent; Liot, Sophie; Prigent, Laura; Alcaraz, Lindsay B.; Verrier, Bernard; Terreux, Raphaël; Moali, Catherine; Lambert, Elise; Valcourt, Ulrich

doi:10.3389/fimmu.2021.613438

Cited by 22 publications

(19 citation statements)

References 66 publications

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“…In the present study, we identified a 15-aa peptide (referred to as hTNX-FGFFFF with an aa sequence of GGLRIPFPRDCGEEM) located at the N-terminal part of the TNX-FG domain as the minimum region responsible for the induction of COL1A1 expression. Interestingly, this minimum region in the TNX-FG domain was not overlapped with some residues in loop 9 in the TNX-FG domain reported by Aubert et al (43), indicating that the 15-aa peptide would fail to interact directly with LAP and mature TGF-β1. However, the fact that SB525334 weakly suppresses the induction of COL1A1 expression with overexpression of hTNX-FGFFFF and integrin α11β1 as shown in Fig.…”

Section: Discussionmentioning

confidence: 65%

COL1A1 expression induced by overexpression of both a 15‑amino acid peptide from the fibrinogen domain of tenascin‑X and integrin α11 in LX‑2 cells

et al. 2022

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Extracellular matrix tenascin-X (TNX) is the largest member of the tenascin family. Our previous study demonstrated that TNX was involved in hepatic dysfunction, including fibrosis, in mice that were administered a high-fat and high-cholesterol diet with high levels of phosphorus and calcium. The present study investigated whether overexpression of both the fibrinogen domain of TNX (TNX-FG) and integrin α11, one of the TNX cell surface receptors, induces in vitro fibrosis in LX-2 human hepatic stellate cells. Overexpression of both a 15-amino acid peptide (hTNX-FGFFFF) derived from the TNX-FG domain and integrin α11 induced the expression of type I collagen α1 chain (COL1A1). Treatment with verteporfin [YAP (Yes-associated protein) inhibitor] attenuated the elevated COL1A1 expression elicited by overexpression of both hTNX-FGFFFF and integrin α11. In addition, small interfering RNA-mediated knockdown of YAP1 resulted in a decrease in COL1A1 expression induced by overexpression of both hTNX-FGFFFF and integrin α11. These results indicated that overexpression of both hTNX-FGFFFF and integrin α11 induced COL1A1 expression via the YAP signaling pathway.

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Section: Discussionmentioning

confidence: 65%

COL1A1 expression induced by overexpression of both a 15‑amino acid peptide from the fibrinogen domain of tenascin‑X and integrin α11 in LX‑2 cells

et al. 2022

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“…It is comprised of 200 kDa hexamers and possesses 511 isoforms, since it contains nine splice variable Fn III domains in addition to the eight constant ones, and a C-terminal FBG-like domain ( 96 ). The FBG domains, highly conserved among the Tenascin family members (TNC, tenascin R, tenascin W, and tenascin X), can dock with TGF-β small latent complex and activate latent TGF-β ( 97 ). In addition to sharing domains that can be unfolded by cell forces with Fn, TNC can bind Fn directly ( 98 ).…”

Section: Hemostasis and Ecmmentioning

confidence: 99%

The interplay of fibroblasts, the extracellular matrix, and inflammation in scar formation

Moretti

Stalfort

Barker

et al. 2022

Journal of Biological Chemistry

123

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Various forms of fibrosis, comprising tissue thickening and scarring, are involved in 40% of deaths across the world. Since the discovery of scarless functional healing in fetuses prior to a certain stage of development, scientists have attempted to replicate scarless wound healing in adults with little success. While the extracellular matrix (ECM), fibroblasts, and inflammatory mediators have been historically investigated as separate branches of biology, it has become increasingly necessary to consider them as parts of a complex and tightly regulated system that becomes dysregulated in fibrosis. With this new paradigm, revisiting fetal scarless wound healing provides a unique opportunity to better understand how this highly regulated system operates mechanistically. In the following review, we navigate the four stages of wound healing (hemostasis, inflammation, repair, and remodeling) against the backdrop of adult versus fetal wound healing, while also exploring the relationships between the ECM, effector cells, and signaling molecules. We conclude by singling out recent findings that offer promising leads to alter the dynamics between the ECM, fibroblasts, and inflammation to promote scarless healing. One factor that promises to be significant is fibroblast heterogeneity and how certain fibroblast subpopulations might be predisposed to scarless healing. Altogether, reconsidering fetal wound healing by examining the interplay of the various factors contributing to fibrosis provides new research directions that will hopefully help us better understand and address fibroproliferative diseases, such as idiopathic pulmonary fibrosis, liver cirrhosis, systemic sclerosis, progressive kidney disease, and cardiovascular fibrosis.

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“…As such, most of the TGF-β deposited in the extracellular space is inactive, although active TGF-β is observed in specific locations ( Barcellos-Hoff et al, 1994 ). Bioavailability of TGF-β is additionally regulated by TGF-β-binding proteins like fibromodulin and decorin which sequester TGF-β and prevent it from binding to specific TGF-β receptors ( Hinz, 2015 ; Khan and Marshall, 2016 ; Nastase et al, 2018 ; Aubert et al, 2021 ). Activation of latent TGF-β is a key step in the regulation of TGF-β-signaling activity.…”

Section: Transforming Growth Factor-β Signaling: Pathways and Mechanismsmentioning

confidence: 99%

Transforming Growth Factor-β: An Agent of Change in the Tumor Microenvironment

Stuelten

Zhang

2021

Front. Cell Dev. Biol.

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Transforming Growth Factor-β (TGF-β) is a key regulator of embryonic development, adult tissue homeostasis, and lesion repair. In tumors, TGF-β is a potent inhibitor of early stage tumorigenesis and promotes late stage tumor progression and metastasis. Here, we review the roles of TGF-β as well as components of its signaling pathways in tumorigenesis. We will discuss how a core property of TGF-β, namely its ability to change cell differentiation, leads to the transition of epithelial cells, endothelial cells and fibroblasts to a myofibroblastoid phenotype, changes differentiation and polarization of immune cells, and induces metabolic reprogramming of cells, all of which contribute to the progression of epithelial tumors.

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Latent TGF-β Activation Is a Hallmark of the Tenascin Family

Cited by 22 publications

References 66 publications

COL1A1 expression induced by overexpression of both a 15‑amino acid peptide from the fibrinogen domain of tenascin‑X and integrin α11 in LX‑2 cells

COL1A1 expression induced by overexpression of both a 15‑amino acid peptide from the fibrinogen domain of tenascin‑X and integrin α11 in LX‑2 cells

The interplay of fibroblasts, the extracellular matrix, and inflammation in scar formation

Transforming Growth Factor-β: An Agent of Change in the Tumor Microenvironment

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